Your Perfect Assignment is Just a Click Away
We Write Custom Academic Papers

100% Original, Plagiarism Free, Customized to your instructions!

glass
pen
clip
papers
heaphones

Discussion: Depression Gin S Malhi, J John Mann

Discussion: Depression Gin S Malhi, J John Mann

Depression Gin S Malhi, J John Mann

Major depression is a common illness that severely limits psychosocial functioning and diminishes quality of life. In 2008, WHO ranked major depression as the third cause of burden of disease worldwide and projected that the disease will rank first by 2030.1 In practice, its detection, diagnosis, and management often pose challenges for clinicians because of its various presentations, unpredictable course and prognosis, and variable response to treatment.

Epidemiology Prevalence The 12-month prevalence of major depressive disorder varies considerably across countries but is approximately 6%, overall.2 The lifetime risk of depression is three times higher (15–18%),3 meaning major depressive disorder is common, with almost one in five people experiencing one episode at some point in their lifetime. Hence, in primary care, one in ten patients, on average, presents with depressive symptoms,4 although the prevalence of depression increases in secondary care settings. Notably, the 12-month prevalence of major depressive disorder is similar when comparing high- income countries (5?5%) with low-income and middle- income countries (5?9%), indicating that major depressive disorder is neither a simple consequence of modern day lifestyle in developed countries, nor poverty.5,6 Furthermore, although social and cultural factors,7 such as socioeconomic status, can have a role in major depression, genomic and other underlying biological factors ultimately drive the occurrence of this condition.8 The most probable period for the onset of the first episode of major depression extends from mid- adolescence to mid-40s, but almost 40% experience their first episode of depression before age 20 years, with an average age of onset in the mid-20s (median 25 years [18–43]).9,10 Across the lifespan, depression is almost twice as common in women than in men and, in both genders, a peak in prevalence occurs in the second and third decades of life, with a subsequent, more modest peak, in the fifth and sixth decades.2,11–13 The difference in prevalence of depression between men and women is referred to as the gender gap in depression and is thought to be linked to sex differences in susceptibility (biological and psychological), and environmental factors that operate on both the microlevel and macrolevel.14

Course and prognosis The onset of depression is usually gradual, but it can be abrupt sometimes, and depression’s course throughout life varies considerably. For most patients, the course of illness is episodic, and they feel well between acute depressive episodes. However, the illness is inherently unpredictable and, therefore, the duration of episodes, the number of episodes over a lifetime, and the pattern in which they occur are variable. Major depressive disorder is a recurrent lifelong illness and so recovery is

somewhat of a misnomer. In practice, the term is used to describe patients that are no longer symptomatic and have regained their usual function following an episode of major depression. With treatment, episodes last about 3–6 months, and most patients recover within 12 months.15 Long-term stable recovery is more probable in community settings and among those patients seen by general physicians than in hospital settings.16 Longer- term (2–6 years), the proportion of people who recover is much less, dropping to approximately 60% at 2 years, 40% at 4 years, and 30% at 6 years with comorbid anxiety having a key role in limiting recovery.17 The likelihood of recurrence is high, the risk increases with every episode, and, overall, almost 80% of patients experience at least one further episode in their lifetime.18,19 The probability of recurrence increases with each episode and the outcome is less favourable with older age of onset.20 Furthermore, although more than half of those affected by a major depressive episode recover within 6 months, and nearly three-quarters within a year, a substantial proportion (up to 27%) of patients do not recover and go on to develop a chronic depressive illness, depending upon baseline patient characteristics and the setting within which they are managed.21,22

Diagnosis The two main classificatory diagnostic systems (Diag- nostic and Statistical Manual of Mental Disorders [DSM],23

Lancet 2018; 392: 2299–312

Published Online November 2, 2018 http://dx.doi.org/10.1016/ S0140-6736(18)31948-2

Department of Academic Psychiatry, Sydney Medical School Northern, University of Sydney, Sydney, NSW, Australia (Prof G S Malhi MD); CADE Clinic, Royal North Shore Hospital, Sydney, NSW, Australia (Prof G S Malhi); and Molecular Imaging and Neuropathology Division, Department of Psychiatry, Columbia University, New York, NY, USA (Prof J J Mann MD)

Correspondence to: Prof Gin S Malhi, Sydney Medical School, University of Sydney, Sydney, NSW 2065, Australia. [email protected]

Search strategy and selection criteria

We searched PubMed for studies published between Jan 1, 2010, and Jan 1, 2018, with the terms “depression”, “depressive disorder”, and “depressive disorder, major”, with specifiers “therapy” and “drug therapy”, as well as “antidepressive agents” and “psychotherapy”. The search excluded articles on depression in the context of bipolar disorder, other psychiatric illnesses (such as schizophrenia), and medical illnesses. We restricted the search to English language publications and focused on publications from the past 5 years. We referred to older publications in the field, especially those regarded as seminal and those that have been highly cited. The search was updated in the periods March 12–16, 2018, and then again July 2–7, 2018, and the bibliographies of selected articles were also reviewed to retrieve publications deemed to be relevant to this Seminar.

http://crossmark.crossref.org/dialog/?doi=10.1016/S0140-6736(18)31948-2&domain=pdf
Seminar

2300 www.thelancet.com Vol 392 November 24, 2018

and International Classification of Diseases [ICD]24) rely on the identification of a number of key symptoms (figure 1). Notably, none of the symptoms are patho gnomonic of depression, and do feature in other psychi atric and medical illnesses. Therefore, the de finition of depression as a disorder is based on symptoms forming a syndrome and causing functional impair ment. Some symptoms are more specific to a depressive disorder, such as anhedonia (diminished ability to experience pleasure); diurnal variation (ie, symptoms of depression are worse during certain periods of waking hours); and intensified guilt about being ill. Other symptoms, such as neurovegetative symptoms, including fatigue, loss of appetite or weight, and insomnia, are very common in other medical illnesses.25

Both taxonomies, DSM and ICD, are widely used to diagnose major depressive disorder within hospital, outpatient, and community settings, but for research, DSM is the predominant classificatory system. In addition to DSM and ICD checklists, the severity of major depression can be quantified with rating scales. Therefore, screening tools have been developed to help

identify depression in various clinical settings, and some that rely on self-report can be used in a waiting room or online.26 However, several screening limitations need to be considered. One limitation is the absence of hierarchy among the range of symptoms that span several domains (emotional, cognitive, and neurovegetative), and which symptoms, if any, warrant priority or greater weighting is unclear. The only symptoms given some primacy are those nominated as fundamental, whereas the remainder carry equal significance (figure 1). In practice, this absence of prioritisation means that very different clinical presentations can qualify as having a depressive syndrome of seemingly equivalent severity, even though the clinical significance of the different presentations can vary markedly.27

In DSM-5, major depressive disorders are separated from bipolar disorders, with the key distinction that manic symptoms only occur in bipolar disorders.28 Major depressive disorder is the principal form of depression and is characterised by recurrent depressive episodes. The diagnosis can be made after a single episode of depression that has lasted two weeks or longer. If episodes of depression do not resolve and last for extended periods of time, this pattern is described as chronic depression. If depressive symptoms are present (on most days) for at least 2 years without any periods of remission exceeding 2 months, the condition is termed persistent depressive disorder or dysthymia.

It is crucial to note that major depressive disorder is different from unhappiness or typical feelings of sadness. To qualify as major depression, an individual must present with five or more specified symptoms (figure 1) nearly every day during a 2-week period, and the symptoms are clearly different from the individual’s previous general function ing. Furthermore, for the diagnosis of a depressive episode, depressed mood or anhedonia must be present.23 When depressive symptoms are present but are insuf cient in number or severity to be regarded as a syndrome, they are sometimes referred to as subthreshold depressive symptoms. These are important as they could serve as early indicators of a major depressive episode.

The symptoms of depression can be broadly grouped into emotional, neurovegetative, and cognitive sym- ptoms, but because they also commonly occur in other psychiatric disorders and medical diseases, detection of a depressive syndrome can be difcult. Some depressive symptoms, such as diminished concentration and psychomotor agitation, are similar to those of mania, and so, when formulating a diagnosis of depression, the possibility of an emerging bipolar disorder warrants consideration.29,30 At the same time, it is important to ensure that the symptoms of depression cannot be explained by an alternative psychiatric diagnosis, such as an anxiety disorder, schizophrenia, or a medical illness, or the side-effects of a medication. Anxiety is

Figure 1: Defining major depressive disorder Key symptoms of Diagnostic and Statistical Manual of Mental Disorders (DSM)-5 for major depressive disorder. For a diagnosis of major depressive disorder, the individual needs to present with five or more of any of the symptoms nearly every day during the same 2-week period, provided at least one of these symptoms is a fundamental one. The clinical symptoms of major depressive disorder are usually accompanied by functional impairment. The greater the number and severity of symptoms (as opposed to particular symptoms), the greater the probability of the functional impairment they are likely to confer. The symptoms of depression can be grouped into emotional, neurovegetative, and neurocognitive domains. Importantly sleep, weight, and appetite are usually diminished in depression but can also be increased, and suicidal ideation, plans, or an attempt should be documented whenever depression is suspected.

Symptoms of depression (2 weeks)

Cumulative functional impairment

Fundamental symptoms Emotional symptoms Neurovegetative symptoms Neurocognitive symptoms

Sleep or

Depressed mood

Fatigue or loss of energy

Ability to think or concentrate, or indecisiveness

Psychomotor retardation or agitation

Anhedonia

Feelings of worthlessness or guilt

Suicidal ideation, plan, or attempt

Weight or appetite or

Seminar

www.thelancet.com Vol 392 November 24, 2018 2301

common in the context of depression, and almost two- thirds of individuals with major depressive disorder have clinical anxiety.31 Anxiety symptoms often appear 1 year or 2 years ahead of the onset of major depression,32 and with increasing age, become a more pronounced feature of major depressive episodes. Therefore, anxiety can manifest both as comorbidity and as a predominant feature of major depressive disorder, sometimes termed anxious depression and described in DSM-5 as an anxious distress specifier (figure 2).33 Of note, depressive symptoms overlap considerably with those of bereave- ment,34 but if the symptoms of depression are severe and persist well beyond the acute grieving period, then consideration should be given to a separate diagnosis of major depressive disorder.35 Alternatively, a diagnosis of adjustment disorder should be considered when the symptoms do not represent typical bereavement but have arisen in response to an identifiable stressor (within 3 months of the onset of the stressor), or the symptoms produce dispro portionately marked distress that results in functional impairment but do not meet the criteria of a major depressive episode. This diagnosis can occur with either depressed mood, anxiety, or both.23 Imp ortantly, stressors are common in both major depressive disorder and adjustment disorder, and therefore stressors are not useful for distinguishing these diagnoses. The key differences are severity and diagnostic criteria of a major depressive episode.

Specifiers and subtypes In practice, it is useful to define the character of each depressive episode, particularly the current or most recent period of illness. This definition is achieved by use of specifiers, which define the pattern of illness, its clinical features (both signs and symptoms), severity, time of onset, and whether it has remitted (figure 2).4,35,36 Some of the clinical features generate putative subtypes

of major depressive disorder. For example, the specifier with melancholic features—ie, a diminished reac- tivity of affect and mood, a pervasive and distinct quality of depressed mood that is worse in the morning, along with anhedonia, guilt, and psychomotor dis- turbance—denotes a melancholic subtype. Such subtyping is some times helpful and it might have potential treatment implications.37 Melancholia is generally more responsive to pharmacotherapy and electroconvulsive therapy. Similarly, major depressive disorder with psychotic features (psychotic depression) often responds best to electroconvulsive therapy, especially when the psychotic features are mood- congruent—ie, feature depressive themes concerning death, loss, illness, and punish ment.38,39 Sometimes, alongside psychotic features, patients can have marked psychomotor disturbance40 and other symptoms that reflect catatonia.41 These subtypes of major depressive disorder are uncommon and most presentations of depression in the community involve symptoms of anxiety,42 described as anxious distress.43 Such presentations are less responsive to antidepressants, even though antidepressants are often used to treat anxiety disorders, suggesting that admixtures of anxiety and depressive symptoms probably reflect additional under lying psychological factors, such as those per- taining to an individual’s personality. Characterising depression in this manner is often helpful, and the use of specifiers to describe depressive episodes in greater detail is good practice that should be routine and adopted more widely.

Detection and screening Depression can manifest in many forms with different combinations of symptoms, which makes its detection more difcult, especially in the context of other illnesses. This mix of symptoms could also explain why depression is often missed or misdiagnosed in primary

Figure 2: Major depressive disorder specifiers Episodes of major depression can be described in greater depth by specifiers (outlined in Diagnostic and Statistical Manual of Mental Disorders-5) that provide additional information regarding the pattern of the illness and its clinical features. Specifiers can also indicate the severity of the episode, when it first emerged (onset), and whether it has remitted (status). For example, in clinical practice, a typical episode of depression can be described as suffering from a recurrence of depression that is moderately severe with melancholic features and has partly remitted in response to initial treatment.

1 Illness pattern

Single episode

Recurrent episode

Rapid cycling

Seasonal

5 Remission status

4 Onset

3 Severity

2 Clinical features

Anxious distress

Mixed features

Atypical

Melancholic

Catatonic

Psychotic

Early

Late

Post partum

Mild

Moderate

Severe

Mild

Moderate

Severe

Mood congruent

Mood incongruent

Partial

Full

Major depressive disorder specifiers

Seminar

2302 www.thelancet.com Vol 392 November 24, 2018

care.27 Greater aware ness of depression increases its successful diagnosis, but screening for depressive illness at a population level has been problematic, which makes its overall detection and diagnosis more difcult.26,44 A substantial proportion of depression probably goes undetected and undiagnosed, and hence published statistics do not fully reflect the burden of the illness. The reasons for this lack of detection are complex and vary across cultures and different health systems, and alongside failures in detection and diagnosis, stigma is an important factor that has been difcult to quantify.45 Case-finding tools that can be used to identify depression are popular among clinicians, such as the nine-item Patient Health Questionnaire (PHQ-9), which comes in three forms, all of which are brief and generally acceptable to patients.46 Such tools can usefully guide detection and the assessment of severity, but it is important that clinicians also assess contextual factors and general functioning, and do not rely solely on questionnaires. Given the prevalence of depression in primary care, routinely asking all patients about mood, interest, and anhedonia since the last visit is essential,47 and when more detailed screening is needed, the burden of administering questionnaires can be limited by the use of computerised adaptive testing methods.48 In addition to enhancing detection through screening, the diagnosis and treatment of major depression can be improved through educational programmes that have great effect on suicide prevention methods.49 However, as shown by a study in Gotland, Sweden, the turnover of doctors due to a 2-year term of service contributed to the requirement for a refresher programme on depression.50 Moreover, attrition in knowledge occurs because once no longer engaged in an educational programme, the general practitioner’s attention shifts to other medical conditions. Therefore, sustaining change in practice requires ongoing education.

Pathology Understanding of the pathophysiology of major depressive disorder has progressed considerably, but no single model or mechanism can satisfactorily explain all aspects of the disease. Different causes or pathophysiology might underlie episodes in different patients, or even different episodes in the same patient at different times. Psychosocial stressors and biological stressors (eg, post-partum period) can result in different pathogenesis and respond preferentially to different interventions. Investigations into the neurobiology of depression have also involved extensive animal research, but extrapolation from animal models of depression and the translation of findings from basic science into clinical practice has proven difcult.51 Therefore, to understand the patho physiology of major depressive disorder, focusing on mechanisms informed directly by clinical studies and examining both

biological and psychosocial factors can be more useful, noting that contributions from these factors are variable.

The monoamine hypothesis The observation, in mid-20th century, that the anti- hypertensive reserpine could trigger major depression and reduce the amount of monoamines, caused interest in the potential role of monoamine neurotransmitters (serotonin, noradrenaline, and dopamine) in the patho- genesis of major depressive disorder. The mono amine theory of major depressive disorder was supported by findings that tricyclic antidepressants and monoamine oxidase inhibitors (MAOIs) enhanced monoamine neuro transmission by different mechanisms, suggesting that this theory explained how anti depressants work (appendix).52 This model has endured, partly because of ongoing corroborative findings from studies that have examined the neurotransmitters and their metabolites, both in vivo and post mortem. The model also endured because other, more selective medi cations, such as auto- receptor antagonists (eg, mirta zapine for the adrenergic system) and serotonin agonists (eg, gepirone), are clinically effective anti depressants.53 However, this model does not explain the notable variability in the clinical presentation of major depressive episodes, even within the same patient, and why some patients respond to one type of antidepressant and others do not. Importantly, this model does not explain why antidepressants take weeks to work.54

Hypothalamic–pituitary–adrenal axis changes The hypothalamic–pituitary–adrenal (HPA) axis has been the focus of depression research for many decades.55–57 One of the most consistent biological findings in more severe depression with melancholic features, and associated with changes in the HPA axis, is the increased amount of plasma cortisol. This biological difference is due to a combination of excessive stress-related cortisol release and impaired glucocorticoid receptor-mediated feedback inhibition. Notably, HPA axis changes are also associated with impaired cognitive function,58 and a failure of HPA axis normalisation with treatment is associated with poor clinical response and high relapse.59 Despite these insights, successful trans lation of this knowledge into clinically effective treatments has not occurred, and treatments that modify HPA axis function, such as glucocorticoid receptor antagonists, have not worked in clinical trials.60–62

Inflammation Peripheral cytokine concentrations have been linked to brain function, wellbeing, and cognition.63 Peripheral cytokines can act directly on neurons and supporting cells, such as astrocytes and microglia, after traversing the blood–brain barrier, or via signals mediated by

See Online for appendix

Seminar

www.thelancet.com Vol 392 November 24, 2018 2303

afferent pathways, such as those in the vagus nerve.64 These mechanisms could explain why individuals with autoimmune diseases and severe infections are more likely to have depression, and why cytokines administered therapeutically, such as interferon gamma and inter leukin 2, trigger depression. The role of inflammation in the causation and exacerbation of depression is further supported by the finding that increased amount of interleukin 6 in childhood enhances the risk of developing depression later in life, and by the evidence of microglial activation and neuroinflammation found in the brains of patients with depression examined post mortem.65 These insights have prompted the examination of non-steroidal anti-inflammatory drugs in the treatment of major depressive disorder.66

Neuroplasticity and neurogenesis One of the most important discoveries in this century has been the identification, in the adult brain, of pluripotent stem cells from which new neurons can be generated, a process termed neurogenesis (appendix). The growth and adaptability at a neuronal level has been more broadly termed neuroplasticity, and it is possibly this neuroplasticity at a cellular level that is altered by inflammation and HPA axis dysfunction, both caused by environmental stress.67 The process of neuro- genesis is controlled by regulatory proteins, such as brain-derived neurotrophic factor (BDNF), which is diminished in patients with major depressive disorder. Even more important, perhaps, is the fact that reduced amounts of BDNF in people with depression can be restored with anti depressant therapies, either pharma- cotherapy or psycho logical interventions.68 In animal studies, limiting neurogenesis prevents antidepressant action and has been shown to result in depression- like symptoms, especially in stressful situations. Therefore, neurogenesis has been suggested to facilitate resilience against stress, which could be the basis of antidepressant clinical effects.69 Post-mortem studies of patients with depression show a deficit of granule neurons in the dentate gyrus of untreated individuals, compared with non-depressed and treated groups. Patients treated for depression have substantially more dividing neuronal progenitor cells compared with an untreated depression group, and even compared with a non-depressed group.70 These findings are consistent with mouse studies showing that anti- depressants can work by increasing neurogenesis in the adult brain.

Structural and functional brain changes Advances in technology and computing over the past quarter of a century have had an immense impact on our understanding of brain structure and function, but meaningful insights have only begun to emerge in the past decade, as it became possible to scan larger numbers of patients and reliably combine neuroimaging data.

Structural studies in patients with depression have consistently found that hippocampal volume is smaller in major depression compared with people without depression,71 and some studies have related the degree of volume loss to duration of untreated lifetime depres- sion.72,73 Post-mortem studies have shown that dentate gyrus volume in untreated patients with depression is about half of that of both a non-depressed comparison group and a group of patients with depression who received treatment.74,75 Whether the smaller hippocampus can be reversed with treatment, and whether it is required for an antidepressant response, is yet to be shown in clinical studies.

Functional neuroimaging provides information about brain networks involved in key processes, such as emotion regulation, rumination, impaired reward pathways related to anhedonia, and self-awareness. Studies examining these networks in depres sive disorders have found that, generally, the amygdala has increased activity and connectivity, and other structures, such as the subgenual anterior cingulate, are hyperactive, but that the insula and dorsal lateral prefrontal cortex are hypoactive, in individuals with depression.76,77 However, the brain changes that have been identified in major depression are related to a highly heterogeneous clinical presentation and, therefore, are also highly variable, making it difcult to replicate results from study to study.78–80 Different types of treatment, such as medication, psychotherapies, and stimulation therapies, have different effects, and research linking pre-existing brain abnormalities to choice of optimal treatment is an area of current research.

Genes Twin and adoption studies have shown that major depressive disorder is moderately heritable.81 First degree relatives of patients with major depression have a three times increase in their risk of developing major depressive disorder compared with those who do not have first degree relatives with a diagnosis of major depression. Unfortunately, reliable identi fication of the genes responsible has proven difcult. So far, genome- wide association studies (GWAS) have identified multiple genes, each with a small effect, and until 2018, few gene hits had been replicated.82 However, current GWAS have begun to successfully identify risk variants and have shown replicable findings that might begin to inform the pathophysiology of major depressive disorder.82–84 Studies that have examined more homo- geneous cases with severe illness also appear promising and have identified loci contributing to risk of major depressive disorder.85 Given the variability of findings, in addition to genomic in vestigations, epigenetic factors are now being examined.

Environmental milieu The potential role of life events in precipitating and possibly causing major depressive disorder has long

Seminar

2304 www.thelancet.com Vol 392 November 24, 2018

been recognised.86,87 For example, early studies examined the impact of stressful life events closely juxtaposed to episodes of major depression, such as preceding its onset by up to a year.88,89 These stressful life events in adults include life threatening or chronic illness, financial difculties, loss of employment, separation, bereavement, and being subjected to violence. The associations between stressful life events and depression have been found to be robust,90,91 though a subgroup of patients seems vulnerable to the effects of stressful life events and another group seems relatively resilient, possibly reflecting biological predispositions. A second approach has examined childhood factors, such as maltreatment including abuse, loss, and neglect, that appear to be associated with a vulnerability to develop major depression during adulthood when confronted with stressful life events.92 By stratifying adversity, such studies have identified at least two types of molecular variants that predispose individuals to major depressive disorder: molecules whose effects depend on adversity and molecules whose effects are present in all cases, irrespective of adversity.93 These studies have identified …

Read more
Applied Sciences
Architecture and Design
Biology
Business & Finance
Chemistry
Computer Science
Geography
Geology
Education
Engineering
English
Environmental science
Spanish
Government
History
Human Resource Management
Information Systems
Law
Literature
Mathematics
Nursing
Physics
Political Science
Psychology
Reading
Science
Social Science
Home
Homework Answers
Blog
Archive
Tags
Reviews
Contact
twitterfacebook
Copyright © 2021 SweetStudy.com

Order Solution Now

Our Service Charter

1. Professional & Expert Writers: Topnotch Essay only hires the best. Our writers are specially selected and recruited, after which they undergo further training to perfect their skills for specialization purposes. Moreover, our writers are holders of masters and Ph.D. degrees. They have impressive academic records, besides being native English speakers.

2. Top Quality Papers: Our customers are always guaranteed of papers that exceed their expectations. All our writers have +5 years of experience. This implies that all papers are written by individuals who are experts in their fields. In addition, the quality team reviews all the papers before sending them to the customers.

3. Plagiarism-Free Papers: All papers provided byTopnotch Essay are written from scratch. Appropriate referencing and citation of key information are followed. Plagiarism checkers are used by the Quality assurance team and our editors just to double-check that there are no instances of plagiarism.

4. Timely Delivery: Time wasted is equivalent to a failed dedication and commitment. Topnotch Essay is known for timely delivery of any pending customer orders. Customers are well informed of the progress of their papers to ensure they keep track of what the writer is providing before the final draft is sent for grading.

5. Affordable Prices: Our prices are fairly structured to fit in all groups. Any customer willing to place their assignments with us can do so at very affordable prices. In addition, our customers enjoy regular discounts and bonuses.

6. 24/7 Customer Support: At Topnotch Essay, we have put in place a team of experts who answer to all customer inquiries promptly. The best part is the ever-availability of the team. Customers can make inquiries anytime.